Tonicity-Responsive Enhancer-Binding Protein Mediates Hyperglycemia-Induced Inflammation and Vascular and Renal Injury

Diabetic nephropathy (DN) has become the single leading cause of ESRD in developed nations. Bearing in mind the paucity of effective treatment for DN and progressive CKD, novel targets for treatment are sorely needed. We previously reported that increased activity of tonicity-responsive enhancer-bin...

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Published in:	Journal of the American Society of Nephrology Vol. 29; no. 2; p. 492
Main Authors:	Choi, Soo Youn, Lim, Sun Woo, Salimi, Shabnam, Yoo, Eun Jin, Lee-Kwon, Whaseon, Lee, Hwan Hee, Lee, Jun Ho, Mitchell, Braxton D, Sanada, Satoru, Parsa, Afshin, Kwon, Hyug Moo
Format:	Journal Article
Language:	English
Published:	United States 01.02.2018
Subjects:	Animals Blood Pressure - genetics Cell Movement Diabetes Mellitus - chemically induced Diabetic Nephropathies - etiology Diabetic Nephropathies - genetics Diabetic Nephropathies - pathology Gene Expression Glomerular Filtration Rate - genetics Haploinsufficiency Humans Hyperglycemia - complications Inflammation - etiology Inflammation - genetics Inflammation - pathology Macrophage Activation - genetics Macrophages - pathology Macrophages - physiology Mice Nitric Oxide Synthase Type III - genetics Polymorphism, Single Nucleotide Renal Insufficiency, Chronic - etiology Renal Insufficiency, Chronic - genetics Renal Insufficiency, Chronic - pathology Streptozocin Transcription Factors - genetics genetic variants blood pressure Diabetic nephropathy chronic kidney disease macrophages
ISSN:	1533-3450, 1533-3450
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Abstract	Diabetic nephropathy (DN) has become the single leading cause of ESRD in developed nations. Bearing in mind the paucity of effective treatment for DN and progressive CKD, novel targets for treatment are sorely needed. We previously reported that increased activity of tonicity-responsive enhancer-binding protein (TonEBP) in monocytes was associated with early DN in humans. We now extend these findings by testing the hypotheses that TonEBP in macrophages promotes hyperglycemia-mediated proinflammatory activation and chronic renal inflammation leading to DN and CKD, and TonEBP genetic variability in humans is associated with inflammatory, renal, and vascular function-related phenotypes. In a mouse model of DN, compared with the wild-type phenotype, TonEBP haplodeficiency associated with reduced activation of macrophages by hyperglycemia, fewer macrophages in the kidney, lower renal expression of proinflammatory genes, and attenuated DN. Furthermore, in a cohort of healthy humans, genetic variants within TonEBP associated with renal function, BP, and systemic inflammation. One of the genetic variants associated with renal function was replicated in a large population-based cohort. These findings suggest that TonEBP is a promising target for minimizing diabetes- and stress-induced inflammation and renovascular injury.
AbstractList	Diabetic nephropathy (DN) has become the single leading cause of ESRD in developed nations. Bearing in mind the paucity of effective treatment for DN and progressive CKD, novel targets for treatment are sorely needed. We previously reported that increased activity of tonicity-responsive enhancer-binding protein (TonEBP) in monocytes was associated with early DN in humans. We now extend these findings by testing the hypotheses that TonEBP in macrophages promotes hyperglycemia-mediated proinflammatory activation and chronic renal inflammation leading to DN and CKD, and TonEBP genetic variability in humans is associated with inflammatory, renal, and vascular function-related phenotypes. In a mouse model of DN, compared with the wild-type phenotype, TonEBP haplodeficiency associated with reduced activation of macrophages by hyperglycemia, fewer macrophages in the kidney, lower renal expression of proinflammatory genes, and attenuated DN. Furthermore, in a cohort of healthy humans, genetic variants within TonEBP associated with renal function, BP, and systemic inflammation. One of the genetic variants associated with renal function was replicated in a large population-based cohort. These findings suggest that TonEBP is a promising target for minimizing diabetes- and stress-induced inflammation and renovascular injury. Diabetic nephropathy (DN) has become the single leading cause of ESRD in developed nations. Bearing in mind the paucity of effective treatment for DN and progressive CKD, novel targets for treatment are sorely needed. We previously reported that increased activity of tonicity-responsive enhancer-binding protein (TonEBP) in monocytes was associated with early DN in humans. We now extend these findings by testing the hypotheses that TonEBP in macrophages promotes hyperglycemia-mediated proinflammatory activation and chronic renal inflammation leading to DN and CKD, and TonEBP genetic variability in humans is associated with inflammatory, renal, and vascular function-related phenotypes. In a mouse model of DN, compared with the wild-type phenotype, TonEBP haplodeficiency associated with reduced activation of macrophages by hyperglycemia, fewer macrophages in the kidney, lower renal expression of proinflammatory genes, and attenuated DN. Furthermore, in a cohort of healthy humans, genetic variants within TonEBP associated with renal function, BP, and systemic inflammation. One of the genetic variants associated with renal function was replicated in a large population-based cohort. These findings suggest that TonEBP is a promising target for minimizing diabetes- and stress-induced inflammation and renovascular injury.Diabetic nephropathy (DN) has become the single leading cause of ESRD in developed nations. Bearing in mind the paucity of effective treatment for DN and progressive CKD, novel targets for treatment are sorely needed. We previously reported that increased activity of tonicity-responsive enhancer-binding protein (TonEBP) in monocytes was associated with early DN in humans. We now extend these findings by testing the hypotheses that TonEBP in macrophages promotes hyperglycemia-mediated proinflammatory activation and chronic renal inflammation leading to DN and CKD, and TonEBP genetic variability in humans is associated with inflammatory, renal, and vascular function-related phenotypes. In a mouse model of DN, compared with the wild-type phenotype, TonEBP haplodeficiency associated with reduced activation of macrophages by hyperglycemia, fewer macrophages in the kidney, lower renal expression of proinflammatory genes, and attenuated DN. Furthermore, in a cohort of healthy humans, genetic variants within TonEBP associated with renal function, BP, and systemic inflammation. One of the genetic variants associated with renal function was replicated in a large population-based cohort. These findings suggest that TonEBP is a promising target for minimizing diabetes- and stress-induced inflammation and renovascular injury.
Author	Salimi, Shabnam Lee-Kwon, Whaseon Lee, Hwan Hee Mitchell, Braxton D Lee, Jun Ho Choi, Soo Youn Parsa, Afshin Kwon, Hyug Moo Lim, Sun Woo Sanada, Satoru Yoo, Eun Jin
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SubjectTerms	Animals Blood Pressure - genetics Cell Movement Diabetes Mellitus - chemically induced Diabetic Nephropathies - etiology Diabetic Nephropathies - genetics Diabetic Nephropathies - pathology Gene Expression Glomerular Filtration Rate - genetics Haploinsufficiency Humans Hyperglycemia - complications Inflammation - etiology Inflammation - genetics Inflammation - pathology Macrophage Activation - genetics Macrophages - pathology Macrophages - physiology Mice Nitric Oxide Synthase Type III - genetics Polymorphism, Single Nucleotide Renal Insufficiency, Chronic - etiology Renal Insufficiency, Chronic - genetics Renal Insufficiency, Chronic - pathology Streptozocin Transcription Factors - genetics
Title	Tonicity-Responsive Enhancer-Binding Protein Mediates Hyperglycemia-Induced Inflammation and Vascular and Renal Injury
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